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1. Serum WFA+-M2 BP is a non-invasive liver fibrosis marker that can predict the efficacy of direct-acting anti-viral-based triple therapy for chronic hepatitis C.

Author

Ura, K., Furusyo, N., Ogawa, E., Hayashi, T., Mukae, H., Shimizu, M., Toyoda, K., Murata, M., and Hayashi, J.

Subjects
WISTERIA, FIBROSIS, NONINVASIVE diagnostic tests, TREATMENT effectiveness, ANTIVIRAL agents, CHRONIC hepatitis C, THERAPEUTICS
Abstract

Background The Wisteria floribunda agglutinin-positive human Mac-2-binding protein ( WFA+-M2 BP) is a new liver fibrosis glycobiomarker with unique fibrosis-related glyco-alteration. WFA+-M2 BP is also a useful surrogate marker for the risk of developing hepatocellular carcinoma and for the liver functional reserve. Aim To evaluate the diagnostic ability of WFA+-M2 BP for liver fibrosis in the clinical setting and the clinical utility of WFA+-M2 BP for predicting the efficacy of direct-acting anti-viral ( DAA) treatment for chronic hepatitis C patients. Methods The study included 159 genotype 1 hepatitis C patients who received DAA-based treatment (telaprevir or simeprevir) combined with pegylated-interferon alpha plus ribavirin (108 telaprevir- and 51 simeprevir-based triple treatment). The relation between baseline serum WFA+-M2 BP and treatment efficacy was evaluated. Results The serum WFA+-M2 BP level significantly increased with the progress of liver fibrosis. Area under the receiver operating characteristic curve analysis identified 2.17 as the cut-off index ( COI) for WFA+-M2 BP for diagnosing advanced fibrosis. The sustained virological response ( SVR) rate was significantly, negatively correlated with the serum WFA+-M2 BP level. Multiple logistic regression analysis found a low serum WFA+-M2 BP level (<2.17 COI) to be independently associated with SVR (odds ratio, 4.35, P = 0.027). Even for prior nonresponders and patients with the interleukin-28B minor allele or histological advanced fibrosis, treatment outcome was favourable for patients with a low serum WFA+-M2 BP level. Conclusion Serum WFA+-M2 BP is a non-invasive liver fibrosis marker useful for predicting the efficacy of DAA-based triple therapy for chronic hepatitis C patients. [ABSTRACT FROM AUTHOR]

Published
2016
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8. Developmental structure of the vertebral column, fins, scutes and scales in bester sturgeon, a hybrid of beluga Huso huso and sterlet Acipenser ruthenus.

Author

Zhang, X., Shimoda, K., Ura, K., Adachi, S., and Takagi, Y.

Subjects
STERLET, FISH development, ANIMAL species, FISH larvae, OSSIFICATION, FISH histology, FISHES, FISH growth, ONTOGENY
Abstract

In the larval bester, a hybrid sturgeon of beluga Huso huso and sterlet Acipenser ruthenus, development of cartilage around the notochord began 7 days post hatch (dph) (14·0 mm, total length, LT). The vertebral cartilage develops in the following sequence: basidorsals and basiventrals, neural canals, neural spines and ribs. The development of ribs remained incomplete in the largest specimen (181 dph, 179 mm LT) that was examined. Endoskeletal development of the fins began 4 dph for the dorsal and anal fins, 6 dph for the pectoral fin and 10 dph for the caudal and pelvic fins. Complete elements of all fins were observed by 91 dph and complete ossification of fin rays was observed by 122 dph in the double-stained specimens. Observation of the histological sections, however, suggested that ossification occurred soon after the formation of the organic matrix in the fin rays. Dorsal scutes were first visible by 25 dph, followed by the lateral and ventral scutes, which were visible by 37 and 44 dph, respectively. The number of scutes was fixed at 44, 59 and 91 dph and ossification was complete by 59 (dorsal) and 91 dph (lateral and ventral scutes) in the double-stained specimens. Ossification occurred soon after the formation of the scute organic matrix in the histological sections. Four types of scales were observed in the H. huso× A. ruthenus hybrid. Median predorsal, preanal and small scales on the anterior section of the head were visible by 59 dph. Scales on the caudal fin were visible by 91 dph and a variable assemblage of scales anterior to the anal fin was visible by 122 dph. Both the scutes and scales developed in a process that is similar to that of intramembranous ossification. [ABSTRACT FROM AUTHOR]

Published
2012
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14. Less protease-resistant PrP in a patient with sporadic CJD treated with intraventricular pentosan polysulphate.

Author

Terada, T., Tsuboi, Y., Obi, T., Doh-ura, K., Murayama, S., Kitamoto, T., Yamada, T., and Mizoguchi, K.

Subjects
ARTERIAL injuries, DISEASES in women, NEUROLOGY, NEUROLOGICAL disorders, HEMORRHAGE
Abstract

Terada T, Tsuboi Y, Obi T, Doh-ura K, Murayama S, Kitamoto T, Yamada T, Mizoguchi K. Less protease-resistant PrP in a patient with sporadic CJD treated with intraventricular pentosan polysulphate. Acta Neurol Scand: 2010: 121: 127–130. © 2009 The Authors Journal compilation © 2009 Blackwell Munksgaard. Treatment with intraventricular pentosan polysulphate (PPS) might be beneficial in patients with Creutzfeldt–Jakob disease. We report a 68-year-old woman with sporadic Creutzfeldt–Jakob disease who received continuous intraventricular PPS infusion (1–120 μg/kg/day) for 17 months starting 10 months after the onset of clinical symptoms. Treatment with PPS was well tolerated but was associated with a minor, transient intraventricular hemorrhage and a non-progressive collection of subdural fluid. The patient’s overall survival time was well above the mean time expected for the illness but still within the normal range. Post-mortem examination revealed that the level of abnormal protease-resistant prion protein in the brain was markedly decreased compared with levels in brains without PPS treatment. These findings suggest that intraventricular PPS infusion might modify the accumulation of abnormal prion proteins in the brains of patients with sporadic Creutzfeldt–Jakob disease. [ABSTRACT FROM AUTHOR]

Published
2010
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15. Fatal acute respiratory distress syndrome after stem cell infusion.

Author

Imataki, O., Ura, K., and Uemura, M.

Subjects
STEM cell transplantation, DYSPNEA, DIURETICS, THERAPEUTICS
Abstract

The article presents a case study of an old lady with transfused acute respiratory distress syndrome (ARDS) developed after stem cell transplantation (SCT) for triggering transfusion-related acute lung injury (TRALI). Topics discussed include experiencing dyspnoea by patient on first day of stem cell transfusion, failure of all interventions including diuretics and catecholamines, and occurrence of TRALI in response to an infused trigger element.

Published
2016
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16. Disease-specific expression of VEGF and its receptors in AML cells: possible autocrine pathway of VEGF/type1 receptor of VEGF in t(15;17) AML and VEGF/type2 receptor of VEGF in t(8;21) AML.

Author

Hi˙ramatsu, A., Mi˙wa, H., Shi˙kami˙, M., Ikai˙, T., Taji˙ma, E., Yamamoto, H., Imai˙, N., Hattori˙, A., Kyo, T., Watarai˙, M., Mi˙ura, K., Satoh, A., Itoh, M., Imamura, A., Mi˙hara, H., Katoh, Y., and Ni˙tta, M.

Subjects
VASCULAR endothelial growth factors, CYTOKINES, PEPTIDES, MESSENGER RNA, CELL culture
Abstract

Various angiogenic factors, such as vascular endothelial growth factor (VEGF) and an associated molecule, placenta growth factor (PlGF), are thought to be important for normal and malignant hematopoiesis. This study examined mRNA expression of VEGF, PlGF and receptors for these molecules in AML cells and identified the disease-specific patterns of expression. AML M 3 having t(15;17) abnormality showed highest expression of VEGF and VEGF receptor type 1 (VEGFR1), suggesting the autocrine pathway of VEGF-VEGFR1. Then, t(8;21) AML demonstrated augmented expression of VEGF and VEGF receptor type 2 (VEGFR2), suggesting VEGF-VEGFR2 autocrine pathway. Then, addition of VEGFR2 kinase inhibitor in Kasumi-1, a t(8;21) AML cell line, resulted in marked inhibition of cell growth, although growth inhibitory effect of R2 kinase inhibitor to HL-60 was marginal. In addition, cell cycle analysis study showed S-phase cell population reduction by R2 kinase inhibitor in Kasumi-1, but not in HL-60. This observation is thought to be the rationale for novel molecular target therapy directed to angiogenic molecules. [ABSTRACT FROM AUTHOR]

Published
2006
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17. Fatal familial insomnia with an unusual prion protein deposition pattern: an autopsy report with an experimental transmission study.

Author

Sasaki, K., Doh-ura, K., Wakisaka, Y., Tomoda, H., and Iwaki, T.

Subjects
INSOMNIA, SLEEP deprivation, SLEEP disorders, GENETIC disorders, PRION diseases, FORENSIC medicine, CEREBRAL cortex, NEUROLOGICAL disorders, GENETIC polymorphisms
Abstract

K. Sasaki, K. Doh-ura, Y. Wakisaka, H. Tomoda and T. Iwaki (2004)Neuropathology and Applied Neurobiology, doi: 10.1111/j.1365-2990.2004.00592.xFatal familial insomnia with an unusual prion protein deposition pattern: an autopsy report with an experimental transmission studyWe recently performed apost-mortemexamination on a Japanese patient who had a prion protein gene mutation responsible for fatal familial insomnia (FFI). The patient initially developed cerebellar ataxia, but finally demonstrated insomnia, hyperkinetic delirium, autonomic signs and myoclonus in the late stage of the illness. Histological examination revealed marked neuronal loss in the thalamus and inferior olivary nucleus; however, prion protein (PrP) deposition was not proved in these lesions by immunohistochemistry. Instead, PrP deposition and spongiform change were both conspicuous within the cerebral cortex, whereas particular PrP deposition was also observed within the cerebellar cortex. The abnormal protease-resistant PrP (PrPres) molecules in the cerebral cortex of this case revealed PrPres type 2 pattern and were compatible with those of FFI cases, but the transmission study demonstrated that a pathogen in this case was different from that in a case with classical FFI. By inoculation with homogenate made from the cerebral cortex, the disease was transmitted to mice, and neuropathological features that were distinguishable from those previously reported were noted. These findings indicate the possibility that a discrete pathogen was involved in the disease in this case. We suggest that not only the genotype of the PrP gene and some other as yet unknown genetic factors, but also the variation in pathogen strains might be responsible for the varying clinical and pathological features of this disease. [ABSTRACT FROM AUTHOR]

Published
2005
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20. An atypical case of sporadic Creutzfeldt–Jakob disease with Parkinson's disease.

Author

Iida, T., Doh-ura, K., Kawashima, T., Abe, H., and Iwaki, T.

Subjects
PARKINSON'S disease, CREUTZFELDT-Jakob disease
Abstract

We report here an autopsy case of a 64-year-old female with slowly progressive dementia and parkinsonism in a 4-year-long clinical course. Post-mortem examination revealed a severely atrophic brain with spongiform degeneration, neuronal loss and gliosis in the gray matter. Many prion protein plaque deposits were present in the occipital lobe, amygdala and cerebellum. Additionally, Lewy bodies were observed in the brainstem. Prion protein gene analysis of the patient revealed polymorphism at the codon-129 valine heterozygote. This genotype is known to sometimes accompany a missense mutation of the gene in uncommon hereditary prion diseases, but no mutation was found in the open reading frame. Thus, it might be suggested that this case showed simultaneously the features of both sporadic Creutzfeldt-Jakob disease (CJD) with codon-129 valine and Parkinson's disease. However, the predisposing factors for contracting both diseases simultaneously remain to be determined, because the incidence of Parkinson's disease accompanied by CJD is very low. [ABSTRACT FROM AUTHOR]

Published
2001
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26. Role of bile acids in duodenal migrating motor complexes in dogs.

Author

Kajiyama, Yuji, Irie, Makoto, Enjoji, Akihito, Ozeki, Kazuyuki, Ura, Kazuhide, Kanematsu, Takashi, Kajiyama, Y, Irie, M, Enjoji, A, Ozeki, K, Ura, K, and Kanematsu, T

Subjects
DUODENUM physiology, ANIMAL experimentation, ANIMALS, DOGS, GASTROINTESTINAL agents, METABOLISM, PORTAL vein, PHARMACODYNAMICS
Abstract

Previous studies have suggested that enterohepatic circulation of bile acids is essential for regular cycling of duodenal migrating motor complexes (MMCs). The present study was an attempt to clarify the role of bile acids in the enterohepatic circulation system in initiating duodenal MMCs. Seven dogs underwent total external biliary diversion that resulted in the loss of MMCs originating from the duodenum. Sodium ursodeoxycholate (6 mg/kg/hr) was then given either through the portal vein or a peripheral vein, and motility of the gastrointestinal tract was serially recorded. When sodium ursodeoxycholate was given either through the portal vein or a peripheral vein during external biliary diversion, duodenal MMCs restarted. The cyclic change in plasma motilin levels during an MMC cycle as induced by sodium ursodeoxycholate was almost the same as in a normal MMC cycle. Total bile acid concentration in the portal vein changed cyclically with MMC cycles when bile flow was intact but did not change cyclically with MMC cycles restarted by intravenous bile salt infusion. Bile acid stimulation of putative receptors existing between the portal vein and intrahepatic bile ducts may be involved in initiating normal duodenal MMC cycles. [ABSTRACT FROM AUTHOR]

Published
1998
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32. Development of a new 3 MV ultra-high voltage electron microscope at Osaka University.

Author

Takaoka, A, Ura, K, Mori, H, Katsuta, T, Matsui, I, and Hayashi, S

Abstract

A new 3 MV ultra-high voltage electron microscope H-3000 was installed at Osaka University. The basic upgrading points are the enhancement of the accelerating voltage and the full computer control. The scale-up of accelerating voltage from 2 MV to 3 MB has required conceptual innovation and the complete redesign of all parts. This has resulted in a new machine with higher performance and new functions. Here, we report on the new technologies employed in the development of the ultra-HVEM. [ABSTRACT FROM PUBLISHER]

Published
1997
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34. Immunohistochemical study on changes in gill Na+/K+-ATPase α-subunit during smoltification in the wild masu salmon, Oncorhynchus masou.

Author

Ura, K., Mizuno, S., Okubo, T., Chida, Y., Misaka, N., Adachi, S., and Yamauchi, K.

Abstract

Changes in immunoreactivity of Na+/K+-ATPase α-subunit in gill sections of wild masu salmon (Oncorhynchus masou) during the parr-smolt transformation (smoltification) were compared with changes in gill Na+/K+-ATPase specific activity. Gill Na+/K+-ATPase specific activity increased from April and peaked in May. Immunohistochemical analysis, using an antiserum against a synthetic oligopeptide based on the conserved region of the Na+/K+-ATPase α-subunit, revealed that immunoreactivity was confined to chloride cells in the surface layer of primary lamellae and the proximal end of secondary lamellae. The size and number of these cells increased gradually from February to May; however, the number of chloride cells of the secondary lamellae decreased in May. These data suggest that the synthesis of Na+/K+-ATPase and the proliferation of chloride cells occur prior to the elevation of enzyme activity. Moreover, it is likely the proliferation and hypertrophy of chloride cells on primary lamellae prepare smolts for entry into seawater and migration in the ocean. [ABSTRACT FROM AUTHOR]

Published
1997
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40. Gerstmann-Sträussler-Scheinker disease in an Alsatian family: clinical and genetic studies.

Author

Tranchant, C, Doh-ura, K, Warter, J M, Steinmetz, G, Chevalier, Y, Hanauer, A, Kitamoto, T, and Tateishi, J

Subjects
CHROMOSOME abnormalities, COMPARATIVE studies, GENEALOGY, GENES, GENETIC techniques, GENETIC mutation, PRIONS, GERSTMANN-Straussler-Scheinker disease, DIAGNOSIS
Abstract

The clinical progression of Gerstmann-Sträussler-Scheinker disease in a family of Alsatian origin is reported. The age of onset and the duration of evolution were variable. The clinical picture became more complex over the generations: in the first generations, isolated dementia and in later generations a triad of pyramidal, pseudobulbar syndromes and dementia associated with spinal cord and cerebellar features. Prion gene analysis showed that four surviving patients carry double missense changes at codons 117 and 129, identical to those found in one case at necropsy and 10 other healthy members of the family. The missense changes were not found in 100 controls. No member of the family had modification of condons 102, 178, or 200. The lod score suggests linkage between the missense change at codon 117 and Gerstmann-Sträussler-Scheinker disease in this family. [ABSTRACT FROM AUTHOR]

Published
1992
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